Mutagenesis, 2012-09, Vol.27 (5), p.523-532
2012
Details
- Autor(en) / Beteiligte
- Titel
- Genotoxicity profile of fexinidazole: a drug candidate in clinical development for human African trypanomiasis (sleeping sickness)
- Ist Teil von
- Mutagenesis, 2012-09, Vol.27 (5), p.523-532
- Ort / Verlag
- Oxford: Oxford University Press
- Erscheinungsjahr
- 2012
- Link zum Volltext
- Quelle
- Oxford Journals 2020 Medicine
- Beschreibungen/Notizen
- The parasitic disease human African trypanomiasis (HAT), also known as sleeping sickness, is a highly neglected fatal condition endemic in sub-Saharan Africa, which is poorly treated with medicines that are toxic, no longer effective or very difficult to administer. New, safe, effective and easy-to-use treatments are urgently needed. Many nitroimidazoles possess antibacterial and antiprotozoal activity and examples such as tinidazole are used to treat trichomoniasis and guardiasis, but concerns about toxicity including genotoxicity limit their usefulness. Fexinidazole, a 2-substituted 5-nitroimidazole rediscovered by the Drugs for Neglected Diseases initiative (DNDi) after extensive compound mining of public and pharmaceutical company databases, has the potential to become a short-course, safe and effective oral treatment, curing both acute and chronic HAT. This paper describes the genotoxicity profile of fexinidazole and its two active metabolites, the sulfoxide and sulfone derivatives. All the three compounds are mutagenic in the Salmonella/Ames test; however, mutagenicity is either attenuated or lost in Ames Salmonella strains that lack one or more nitroreductase(s). It is known that these enzymes can nitroreduce compounds with low redox potentials, whereas their mammalian cell counterparts cannot, under normal conditions. Fexinidazole and its metabolites have low redox potentials and all mammalian cell assays to detect genetic toxicity, conducted for this study either in vitro (micronucleus test in human lymphocytes) or in vivo (ex vivo unscheduled DNA synthesis in rats; bone marrow micronucleus test in mice), were negative. Thus, fexinidazole does not pose a genotoxic hazard to patients and represents a promising drug candidate for HAT. Fexinidazole is expected to enter Phase II clinical trials in 2012.
- Sprache
- Englisch
- Identifikatoren
- ISSN: 0267-8357eISSN: 1464-3804DOI: 10.1093/mutage/ges015Titel-ID: cdi_proquest_miscellaneous_1069200095
- Format
- –
- Schlagworte
- African trypanosomiasis, Ames test, Animals, Antiprotozoal activity, Bacteria - drug effects, Bacteria - enzymology, Biological and medical sciences, Bone marrow, Bone Marrow Cells - drug effects, Clinical trials, DNA biosynthesis, Drug development, Drugs, Enzymes, Fundamental and applied biological sciences. Psychology, Genotoxicity, Hepatocytes - drug effects, Humans, Leukocytes, Mononuclear - drug effects, Lymphocytes, Male, Mammalian cells, Metabolites, Mice, Micronucleus Tests, Molecular and cellular biology, Molecular genetics, Mutagenesis, Mutagenesis. Repair, Mutagenicity, Mutagenicity Tests, Mutagens - metabolism, Mutagens - toxicity, nitroimidazoles, Nitroimidazoles - metabolism, Nitroimidazoles - toxicity, Nitroreductases - metabolism, Parasitic diseases, Pharmaceuticals, Rats, Redox potential, Salmonella, Tinidazole, Trichomoniasis, Trypanocidal Agents - metabolism, Trypanocidal Agents - toxicity, Trypanosomiasis, African - drug therapy